Hurtado Plinio R, Jeffs Lisa, Nitschke Jodie, Patel Mittal, Sarvestani Ghafar, Cassidy John, Hissaria Pravin, Gillis David, Peh Chen Au
Renal Unit, Royal Adelaide Hospital, North Terrace, Adelaide, 5000, Australia.
BMC Immunol. 2008 Jul 14;9:34. doi: 10.1186/1471-2172-9-34.
Wegener's Granulomatosis and Microscopic Polyangiitis are life-threatening systemic necrotizing vasculitides of unknown aetiology. The appearance of circulating antibodies to neutrophil cytoplasmic antigens (ANCA) is strongly associated with the development of the disease. A link between infection and disease has long been suspected, and the appearance of ANCA antibodies has been reported following bacterial and viral infections. The depletion of circulating B cells with monoclonal antibody therapy can induce remission, and this observation suggests a pathogenic role for B cells in this disease. As bacterial DNA is known to induce B cell proliferation and antibody production via TLR-9 stimulation, we have explored the possibility that unmethylated CpG oligodeoxynucleotide, as found in bacterial and viral DNA, may play a role in stimulating circulating autoreactive B cells to produce ANCA in patients with vasculitis.
We have confirmed that unmethylated CpG oligonucleotide is a potent stimulator of antibody production by PBMC in vitro. The stimulation of PBMC with CpG oligonucleutides resulted in the production of similar amounts of IgG in both ANCA+ patients and normal controls. In spite of this, PR3 ANCA+ patients synthesised significantly higher amount of IgG ANCA than normal controls. In MPO ANCA+ patients, there was a tendency for patients to produce higher amount of ANCA than controls, however, the difference did not reach significance. Furthermore, we were able to detect circulating MPO-reactive B cells by ELISpot assay from the peripheral blood of 2 MPO+ ANCA vasculitis patients. Together, this indicates that circulating anti-neutrophil autoreactive B cells are present in ANCA+ vasculitis patients, and they are capable of producing antibodies in response to CpG stimulation. Of note, CpG also induced the production of the relevant autoantibodies in patients with other types of autoimmune diseases.
Circulating ANCA autoreactive B cells are present in patients with ANCA+ vasculitis. The production of ANCA from these cells in response to unmethylated CpG stimulation lead us to propose that stimulation of these cells by immunostimulatory DNA sequences such as CpG oligodeoxynucleotide during infection may provide a link between infection and ANCA associated vasculitis. This phenomenon may also apply to other antibody mediated autoimmune diseases.
韦格纳肉芽肿病和显微镜下多血管炎是病因不明的危及生命的系统性坏死性血管炎。抗中性粒细胞胞浆抗原(ANCA)循环抗体的出现与疾病的发展密切相关。长期以来人们一直怀疑感染与疾病之间存在联系,并且在细菌和病毒感染后已报道了ANCA抗体的出现。用单克隆抗体疗法清除循环B细胞可诱导缓解,这一观察结果提示B细胞在该疾病中具有致病作用。由于已知细菌DNA通过TLR-9刺激诱导B细胞增殖和抗体产生,我们探讨了在细菌和病毒DNA中发现的未甲基化CpG寡脱氧核苷酸可能在刺激血管炎患者循环自身反应性B细胞产生ANCA中起作用的可能性。
我们已证实未甲基化的CpG寡核苷酸在体外是PBMC抗体产生的有效刺激物。用CpG寡核苷酸刺激PBMC导致ANCA阳性患者和正常对照中产生相似量的IgG。尽管如此,PR3 ANCA阳性患者合成的IgG ANCA量明显高于正常对照。在MPO ANCA阳性患者中,患者产生的ANCA量有高于对照的趋势,然而,差异未达到显著水平。此外,我们能够通过ELISpot测定法从2例MPO阳性ANCA血管炎患者的外周血中检测到循环MPO反应性B细胞。总之,这表明ANCA阳性血管炎患者中存在循环抗中性粒细胞自身反应性B细胞,并且它们能够响应CpG刺激产生抗体。值得注意的是,CpG还诱导其他类型自身免疫性疾病患者产生相关自身抗体。
ANCA阳性血管炎患者中存在循环ANCA自身反应性B细胞。这些细胞响应未甲基化CpG刺激产生ANCA,这使我们提出在感染期间由免疫刺激DNA序列如CpG寡脱氧核苷酸刺激这些细胞可能提供感染与ANCA相关血管炎之间的联系。这种现象也可能适用于其他抗体介导的自身免疫性疾病。
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